Analysis of Pax6 Contiguous Gene Deletions in the Mouse, Mus musculus, Identifies Regions Distinct from Pax6 Responsible for Extreme Small-Eye and Belly-Spotting Phenotypes

Favor, Jack; Bradley, Allan; Conte, Nathalie; Janik, Dirk; Pretsch, Walter; Reitmeir, Peter; Rosemann, Michael; Schmahl, W.; Wienberg, Johannes; Zaus, Irmgard

doi:10.1534/genetics.109.104562

Cited by 15 publications

(10 citation statements)

References 54 publications

(54 reference statements)

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“…A familial case of aniridia resulting from a deletion containing PAX6 , RCN1 , and DKFZp686k1684 was reported by Zhang et al (2011). Severe visual impairment observed in the described family is compatible with the mouse phenotype reported by Favor et al (2009). Patient p9 contains a very similar deletion of the downstream flanking region of PAX6 to the family described by Zhang et al (2011).…”

Section: Discussionsupporting

confidence: 90%

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11p13 deletions can be more frequent than the PAX6 gene point mutations in Polish patients with aniridia

et al. 2013

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Aniridia is a rare, bilateral, congenital ocular disorder causing incomplete formation of the iris, usually characterized by iris aplasia/hypoplasia. It can also appear with other ocular anomalies, such as cataracts, glaucoma, corneal pannus, optic nerve hypoplasia, macular hypoplasia, or ectopia lentis. In the majority of cases, it is caused by mutation in the PAX6 gene, but it can also be caused by microdeletions that involve the 11p13 region. Twelve unrelated patients of Polish origin with a clinical diagnosis of aniridia were screened for the presence of microdeletions in the 11p13 region by means of multiplex ligation probe amplification (MLPA). Additionally, the coding regions of the PAX6 gene were sequenced in all probands. MLPA examination revealed different size deletions of the 11p13 region in five patients. In three cases, deletions encompassed the entire PAX6 gene and a few adjacent genes. In one case, a fragment of the PAX6 gene was deleted only. In the final case, the deletion did not include any PAX6 sequence. Our molecular findings provide further evidence of the existence of the distant 3′ regulatory elements in the downstream region of the PAX6 gene, which is known from other studies to influence the level of protein expression. Sequence analysis of the PAX6 gene revealed the three different point mutations in the remaining four patients with aniridia. All the detected mutations were reported earlier. Based on accomplished results, the great diversity of the molecular basis of aniridia was found. It varies from point mutations to different size deletions in the 11p13 region which encompass partly or completely the PAX6 gene or cause a position effect.

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Section: Discussionsupporting

confidence: 90%

“…The RCN1 gene is a Ca 2+ binding protein, participating in the secretory pathway. Favor et al (2009) reported that mouse, containing a heterozygous deletion of the AX6 and RCN1 genes, presents an extreme microphthalmia. They suggest that RCN1 may have an influence on the eye phenotype in PAX6 contiguous gene deletions.…”

Section: Discussionmentioning

confidence: 99%

11p13 deletions can be more frequent than the PAX6 gene point mutations in Polish patients with aniridia

et al. 2013

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“…This creates an unnatural situation making some phenotypes frail in a way that does not reflect the biology under study and introduces extraneous variables [30, 36]. Finally, environmental variables such as cage conditions, handling practices, and even the experimenter can increase variability [37–39]. Studies of the Sey allele have been conducted on numerous different bkgds and at various timepoints, often focusing on embryonic development.…”

Section: Introductionmentioning

confidence: 99%

Epistasis between Pax6Sey and genetic background reinforces the value of defined hybrid mouse models for therapeutic trials

et al. 2018

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The small eye (Sey) mouse is a model of PAX6-aniridia syndrome (aniridia). Aniridia, a congenital ocular disorder caused by heterozygous loss-of-function mutations in PAX6, needs new vision saving therapies. However, high phenotypic variability in Sey mice makes development of such therapies challenging. We hypothesize that genetic background is a major source of undesirable variability in Sey mice. Here we performed a systematic quantitative examination of anatomical, histological, and molecular phenotypes on the inbred C57BL/6J, hybrid B6129F1, and inbred 129S1/SvImJ backgrounds. The Sey allele significantly reduced eye weight, corneal thickness, PAX6 mRNA and protein levels, and elevated blood glucose levels. Surprisingly, Pax6Sey/Sey brains had significantly elevated Pax6 transcripts compared to Pax6+/+ embryos. Genetic background significantly influenced 12/24 measurements, with inbred strains introducing severe ocular and blood sugar phenotypes not observed in hybrid mice. Additionally, significant interactions (epistasis) between Pax6 genotype and genetic background were detected in measurements of eye weight, cornea epithelial thickness and cell count, retinal mRNA levels, and blood glucose levels. The number of epistatic interactions was reduced in hybrid mice. In conclusion, severe phenotypes in the unnatural inbred strains reinforce the value of more naturalistic F1 hybrid mice for the development of therapies for aniridia and other disorders.

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“…In contrast, Cdh1 was present exclusively on P30 relative to P14, and plays a role in cell-cell adhesions, mobility and proliferation of epithelial cells [ 48 ]. Additional proteins exclusively expressed on P3 relative to P14 include reticulocalbin-1, plexin-B2, and low-density lipoprotein receptor-related protein 2, which are involved in the development of sensory organs [ 49 ] and nervous system [ 50 , 51 ] and thus may contribute to the development of the cochlear sensory epithelium.…”

Section: Discussionmentioning

confidence: 99%

Label-free quantitative mass spectrometry analysis of differential protein expression in the developing cochlear sensory epithelium

Darville

Sokolowski

2018

Proteome Sci

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BackgroundThe sensory epithelium of the inner ear converts the mechanical energy of sound to electro-chemical energy recognized by the central nervous system. This process is mediated by receptor cells known as hair cells that express proteins in a timely fashion with the onset of hearing.MethodsThe proteomes of 3, 14, and 30 day-old mice cochlear sensory epithelia were revealed, using label-free quantitative mass spectrometry (LTQ-Orbitrap). Statistical analysis using a one-way ANOVA followed by Bonferroni’s post-hoc test was used to show significant differences in protein expression. Ingenuity Pathway Analysis was used to observe networks of differentially expressed proteins, their biological processes, and associated diseases, while Cytoscape software was used to determine putative interactions with select biomarker proteins. These candidate biomarkers were further verified using Western blotting, while coimmunoprecipitation was used to verify putative partners determined using bioinformatics.ResultsWe show that a comparison across all three proteomes shows that there are 447 differentially expressed proteins, with 387 differentially expressed between postnatal day 3 and 30. Ingenuity Pathway Analysis revealed ~ 62% of postnatal day 3 downregulated proteins are involved in neurological diseases. Several proteins are expressed exclusively on P3, including Parvin α, Drebrin1 (Drb1), Secreted protein acidic and cysteine rich (SPARC), Transmembrane emp24 domain-containing protein 10 (Tmed10). Coimmunoprecipitations showed that Parvin and SPARC interact with integrin-linked protein kinase and the large conductance calcium-activated potassium channel, respectively.ConclusionsQuantitative mass spectrometry revealed the identification of numerous differentially regulated proteins over three days of postnatal development. These data provide insights into functional pathways regulating normal sensory and supporting cell development in the cochlea that include potential biomarkers. Interacting partners of two of these markers suggest the importance of these complexes in regulating cellular structure and synapse development.Electronic supplementary materialThe online version of this article (10.1186/s12953-018-0144-6) contains supplementary material, which is available to authorized users.

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Analysis of Pax6 Contiguous Gene Deletions in the Mouse, Mus musculus, Identifies Regions Distinct from Pax6 Responsible for Extreme Small-Eye and Belly-Spotting Phenotypes

Cited by 15 publications

References 54 publications

11p13 deletions can be more frequent than the PAX6 gene point mutations in Polish patients with aniridia

11p13 deletions can be more frequent than the PAX6 gene point mutations in Polish patients with aniridia

Epistasis between Pax6Sey and genetic background reinforces the value of defined hybrid mouse models for therapeutic trials

Label-free quantitative mass spectrometry analysis of differential protein expression in the developing cochlear sensory epithelium

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